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腺病毒2型和猿猴病毒40转化的仓鼠细胞分泌的促有丝分裂和抗有丝分裂转化生长因子:在促进肿瘤发生中的可能作用。

Mitogenic and antimitogenic transforming growth factors secreted by adenovirus 2- and simian virus 40-transformed hamster cells: possible roles in promoting tumorigenesis.

作者信息

Akagi K, Murai K, Haddada H, Levine A S, Patch C T

出版信息

Cancer Res. 1987 Aug 1;47(15):4086-92.

PMID:3038307
Abstract

Adenovirus 2 (Ad2)- and simian virus 40 (SV40)-transformed hamster embryo cells differ markedly in a number of phenotypic properties including their potential for inducing tumors in hamsters. Both Ad2- and SV40-transformed cells are immortalized and readily induce tumors in immunoincompetent newborn syngeneic hamsters, but only SV40-transformed cells are highly oncogenic in both adult syngeneic and allogeneic immunocompetent hamsters. The reasons for the difference in the oncogenic potential of the Ad2- and SV40-transformed phenotypes remain elusive. However, recent studies with transforming growth factors (TGFs) indicate that these factors play an important role in determining many phenotypic characteristics of transformed cells. To determine whether TGFs secreted by Ad2- and SV40-transformed hamster embryo cells differ, we have examined the ability of media conditioned by these two transformed cell phenotypes to modulate thymidine uptake in quiescent, untransformed cells. We found that both transformed phenotypes secrete very similar TGF alpha-like mitogenic factors which inhibit binding of 125I-labeled epidermal growth factor to its receptor. Our results also show that SV40-transformed cells, but not Ad2-transformed cells, secrete a powerful mitogenic inhibitor (MI). The MI secreted by SV40-transformed cells is inhibitory for several transformed and untransformed cell types and exerts a cytostatic, not cytolytic, action on untransformed primary hamster embryo cells. MI elutes from size exclusion high-performance liquid chromatography columns with a molecular weight of 24,000. Although MI has about the same molecular weight as TGF beta, it differs from TGF beta in two important respects: it is heat labile and it has a different target specificity for antimitogenic activity. The MI secreted by SV40-transformed cells also inhibits thymidine uptake by concanavalin A-stimulated spleen lymphocytes. This finding suggests that MI might contribute to the extreme oncogenicity of SV40-transformed cells by inhibiting mobilization of immune effector cells at the site of tumor cell proliferation.

摘要

腺病毒2(Ad2)和猴病毒40(SV40)转化的仓鼠胚胎细胞在许多表型特性上有显著差异,包括它们在仓鼠体内诱导肿瘤的潜力。Ad2和SV40转化的细胞都是永生化的,并且很容易在免疫缺陷的同基因新生仓鼠中诱导肿瘤,但只有SV40转化的细胞在成年同基因和异基因免疫 competent 仓鼠中具有高度致癌性。Ad2和SV40转化表型致癌潜力差异的原因仍然难以捉摸。然而,最近关于转化生长因子(TGFs)的研究表明,这些因子在决定转化细胞的许多表型特征中起重要作用。为了确定Ad2和SV40转化的仓鼠胚胎细胞分泌的TGFs是否不同,我们检测了这两种转化细胞表型条件培养基调节静止、未转化细胞中胸苷摄取的能力。我们发现这两种转化表型都分泌非常相似的TGFα样促有丝分裂因子,它们抑制125I标记的表皮生长因子与其受体的结合。我们的结果还表明,SV40转化的细胞,而不是Ad2转化的细胞,分泌一种强大的促有丝分裂抑制剂(MI)。SV40转化细胞分泌的MI对几种转化和未转化的细胞类型具有抑制作用,并对未转化的原代仓鼠胚胎细胞发挥细胞抑制作用,而非细胞溶解作用。MI从分子量排阻高效液相色谱柱上洗脱时的分子量为24,000。虽然MI的分子量与TGFβ大致相同,但它在两个重要方面与TGFβ不同:它对热不稳定,并且在抗有丝分裂活性方面具有不同的靶标特异性。SV40转化细胞分泌的MI还抑制伴刀豆球蛋白A刺激的脾淋巴细胞摄取胸苷。这一发现表明,MI可能通过抑制肿瘤细胞增殖部位免疫效应细胞的动员,导致SV40转化细胞的极端致癌性。

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